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A pharmacological study of NLP-12 neuropeptide signaling in free-living and parasitic nematodes

机译:NLP-12神经肽信号传导在自由生活和寄生线虫中的药理研究

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NLP-12a and b have been identified as cholecystokinin/sulfakinin-like neuropeptides in the free-living nematode Caenorhabditis elegans. They are suggested to play an important role in the regulation of digestive enzyme secretion and fat storage. This study reports on the identification and characterization of an NLP-12-like peptide precursor gene in the rat parasitic nematode Strongyloides ratti. The S. ratti NLP-12 peptides are able to activate both C. elegans CKR-2 receptor isoforms in a dose-dependent way with affinities in the same nanomolar range as the native C. elegans NLP-12 peptides. The C-terminal RPLQFamide sequence motif of the NLP-12 peptides is perfectly conserved between free-living and parasitic nematodes. Based on systemic amino acid replacements the Arg-, Leu- and Phe- residues appear to be critical for high-affinity receptor binding. Finally, a SAR analysis revealed the essential pharmacophore in C. elegans NLP-12b to be the pentapeptide RPLQFamide.
机译:NLP-12a和b已被鉴定为自由活动线虫秀丽隐杆线虫中的胆囊收缩素/磺胺激酶样神经肽。建议它们在调节消化酶分泌和脂肪储存中起重要作用。这项研究报告了大鼠寄生线虫Strongyloides ratti中的NLP-12样肽前体基因的鉴定和表征。鼠链球菌NLP-12肽能够以剂量依赖的方式激活秀丽隐杆线虫CKR-2受体同工型,亲和力与天然秀丽隐杆线虫NLP-12肽相同。 NLP-12肽的C端RPLQFamide序列基序在自由生活线虫和寄生线虫之间是完全保守的。基于系统氨基酸置换,Arg-,Leu-和Phe-残基似乎对高亲和力受体结合至关重要。最后,SAR分析显示秀丽隐杆线虫NLP-12b中必不可少的药效团是五肽RPLQFamide。

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